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Acute leukemia and myelodysplastic syndromes
Peter Vandenberghe
Centrum Menselijke Erfelijkheid &
Afdeling Hematologie, UZ Leuven
Post-ASH meeting 1 11/01/2012
11/01/2012 Post-ASH meeting 2
1. Acute myeloid leukemia
2. Myelodysplastic syndromes
3. Acute lymphoblastic leukemia/lymphoma
Post-ASH meeting 3 11/01/2012
Speck & Gilliland, Nat Rev Cancer. 2002 ;2:502-13
Acute leukemia : two cooperating classes of mutations
22nd General Meeting of the Belgian Hematological Society, 2007
Genetics of AML ~2000
Abnormal cytogenetics Normal cytogenetics
favorable
unfavorable
intermediate intermediate
Contemporary view on the genetic complexity of acute myeloid leukemia
Abnormal cytogenetics Normal cytogenetics
favorable
unfavorable
intermediate
FLT3
KIT
FLT3
NPM1
Adapted from
Döhner H et al. Blood 2010;115:453-474
11/01/2012 5 Post-ASH meeting
Post-ASH meeting 6 11/01/2012
Updated from Speck & Gilliland, Nat Rev Cancer. 2002 ;2:502-13
Acute myeloid leukemia : two cooperating classes of mutations
SNP arrays / Next generation sequencing
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• Next generation sequencing (NGS) / massive parallel sequencing
• Whole genome sequencing
• Exome sequencing
• Transcriptome sequening
• Methylome
• Histon code
• IDH1/IDH2/DNMT3A/ ….
• CGH/SNP arrays
• Gains
• Losses
• LOH
• TET2/EZH2/IKZF1
Recent mutations in CN AML
IDH1 (2q33)/ IDH2 (15q26) : oncometabolites and transformation
• incidence • IDH1 / IDH2 : 15-22%
• TET2 : 12-27%
• Patterns • IDH1 (R132)/ IDH2 (R140)
• IR karyotype, normal karyotype, NPM1 mut
• IDH2 (R172)
• IR karyotype, no other mutations
• Prognosis in CN- AML • TET2 :
• IDH1 R132:
• IDH2 R140:
• IDH2 R172:
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Recent mutations in AML
DNMT3A (2p23), a de novo DNA-methyltransferase
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• Incidence
• adult AML ~17-22 %, ped AML 0% (MDS 10%, T-ALL 10% #407)
• Intermediate risk cytogenetics (never with favorable risk cytogenetics)
• AML-M4-M5, older age, high WBC
• Associated with Flt3-ITD, NPM1 mut, IDH1/2 mut • Heterozygous in myeloid, can be biallelic in lymphoid
• Associated with worse prognosis in multivariate analysis
OS 12.3 mo
• Unresolved: • biomarker for demethylating therapy ?
• Transforming mechanism : increased SC renewal ? (quid role of
FLT3/NPM1 context)
New mutations in AML # 404 Complete Sequencing and Comparison of 12 Normal Karyotype M1 AML Genomes with 12
t(15;17) Positive M3-APL Genomes
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• Whole genome sequencing : CN AML-M1 (n=12), APL (n=12), additional testing in 34 CN-
AML M1 and 9 APL
• Far less mutations compared with solid tumors; #SNV increases with age
New mutations in AML # 404 Complete Sequencing and Comparison of 12 Normal Karyotype M1 AML Genomes with 12
t(15;17) Positive M3-APL Genomes
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• Whole genome sequencing : CN AML-M1 (n=12), APL (n=12), additional testing in 34 CN-AML M1 and 9 APL
n= 22 n=3 n=25
APL AML-M1
Cohesin complex 3
New mutations in AML
# 4 Clonal Evolution of Pre-Leukemic Hematopoietic Stem Cells
Precedes Human Acute Myeloid Leukemia
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Prospective isolation of HSC, LSC, AML
Exome sequencing of AML
Retrieval of mutations in single HSC or LSC
New mutations in AML
#4 Clonal Evolution of Pre-Leukemic Hematopoietic Stem Cells
Precedes Human Acute Myeloid Leukemia
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New mutations in AML
#4 Clonal Evolution of Pre-Leukemic Hematopoietic Stem Cells
Precedes Human Acute Myeloid Leukemia
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New mutations in AML : BECOR (Xp11.4)
# 71 Whole-Exome Sequencing Identifies Recurrent Mutations of BCOR in
Acute Myeloid Leukemia with Normal Karyotype
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• Whole exome sequencing of CN-AML w/o mutations of CEBPA, NPM1, FLT3-ITD or MLL-PTD
• BCOR (BCL6 corepressor, Xp11.4)
• Germline mutations in oculo-facio-cardio-dental syndrome
• Nonsense, frameshift, splice site mutations • in 14/82 cases with CN-AML w/o mutations of CEBPA, NPM1, FLT3-ITD or MLL-PTD
• in 11/262 cases with unselected CN-AML
• never in good risk cytogenetics or CEBPA dm, very rarely with NPM1
• Strongly associated with DNMT3A and RUNX1 mutations
• Associated with poor prognosis (2y OS 28% vs 66 % in CN AML)
Genetics and therapy of AML
• Perspective of personalized diagnosis coming soon but perspective of
personalised therapy remains more remote
• Many new & unexpected driver mutations and pathways discovered
• Heterogeneity of the disease, need for increased accrual in clinical trials
• Development of existing drugs vs. searching new ones ?
• Which strategies to target the LSC ?
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Therapy of AML #6 Fractionated Doses of Gemtuzumab Ozogamicin (GO) Combined to Standard Chemotherapy (CT)
Improve Event-Free and Overall Survival in Newly-Diagnosed De Novo AML Patients Aged 50-70
Years Old: A Prospective Randomized Phase 3 Trial From the Acute Leukemia French Association
(ALFA)
• De novo AML (excluding APL), age 50-70, n = 280
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Therapy of AML # 6 Fractionated Doses of Gemtuzumab Ozogamicin (GO) Combined to Standard Chemotherapy
(CT) Improve Event-Free and Overall Survival in Newly-Diagnosed De Novo AML Patients Aged 50-70
Years Old: A Prospective Randomized Phase 3 Trial From the Acute Leukemia French Association
(ALFA)
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DAGO DA p
N 137 134
CR-CRp 81% 75% 0.31
Early death 9 5 0.41
EFS (30 mo) 41 % 20% 0.0018
Med OS 34 mo 19 mo 0.037
Med RFS 28 mo 12 mo
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• 1. Acute myeloid leukemia
2. Myelodysplastic syndromes
3. Acute lymphoblastic leukemia/lymphoma
Myelodysplastic syndromes # 3 Somatic Mutation of SF3B1 (2q33), a Gene Encoding a Core Component of RNA Splicing
Machinery, in Myelodysplasia with Ring Sideroblasts
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•Whole Exome Sequencing in 9 cases
•64 point mutations
•RNA splicing factor 3B subunit1 mutation
exon12-15) in 72/354 (20%) patients with
MDS, and in 53/82 (65 %) patients with MDS-
RS
•Associated with TET2
•Also found in other malignancies
•Associated with favorable OS and LFS
11/01/2012 Post-ASH meeting 22
• 1. Acute myeloid leukemia
2. Myelodysplastic syndromes
3. Acute lymphoblastic leukemia/lymphoma
Acute lymphoblastic leukemia: how to optimize long term outcome in
adult Ph(+) acute lymphoblastic leukemia ? (Adele Fielding, educational session)
• 25% of adult B-ALL, older population
• Superior CRs with TKI in initial remission induction therapy
• ? How much chemo is required for an optimal long-term response ? Is chemo
required at all ?
• Which TKI ? Increased toxicity with DAS ?
• Postremission therapy : allo-HCT is key for long term outcome in
adults (OS 50-70 % @ 3y in several studies (UKALL12/GMALL/JALSG))
• How much myeloablation is required for optimal long term response ? Myeloablative
versus RIC, with RIC gaining more widespread use
• TKI after alloHCT ?: insufficient evidence for general
recommendation: case by case, qBCR-ABL1 monitoring
11/01/2012 Post-ASH meeting 23
Acute lymphoblastic leukemia: how to improve long term
outcome in other subsets of poor risk ALL ?
• #69 Whole Genome Sequence Analysis of 22 MLL Rearranged Infant Acute Lymphoblastic Leukemias Reveals Remarkably Few Somatic Mutations: A Report From the St Jude Children‘s Research Hospital - Washington University Pediatric
Cancer Genome Project
• MLL rearrangements can be very complex (chromotrypsis), leading to additional in frame fusions
• In addition to MLL rearrangement, very few mutations (on average 4.8 (0-11) lesions/ case) ( RAS pathway, B-cell differentiation
• More mutations in non-infant MLL –R ALL; many more at relapse
• #70 Ras Signalling Pathway and Novel Target Genes Related to Down Syndrome Contribute to the Development of B-Cell
Precursor Acute Lymphoblastic Leukemia (BCP-ALL) in iAMP21 patients (n=1 +44) (exome sequencing)
• # 67 Novel Chromosomal Rearrangements and Sequence Mutations in High-Risk Ph-Like Acute Lymphoblastic
Leukemia (n=12 + 94) (15% of childhood/adolescent B-ALL) with IKZF1 deletions/mutations
• Lesions impairing normal B-cell development (PAX5, EBP, IKZF1, ….)
• Constitutive growth signals
• 40 % IGH-CRLF2 +/- JAK 2 mutations
• EBF-PDGFRA
• STRN3-JAK2
• NUP214-ABL1
• BCR-JAK2
• IGH-EPOR
• IL7R mutations + loss of SH2B3 (link)
• # 68 Discovery of Novel Recurrent Mutations in Childhood Early T-Cell Precursor Acute Lymphoblastic Leukemia
(n=12 +53) by Whole Genome Sequencing
• Complex inter- en intrachromosomal reaargmnts /cytokine receptor and RAS/B-T developmental genes/ EZH2 and PRC2
• similarities with AML
• # 403 The Genomic Landscape of TEL-AML1+ (ETV6-RUNX1) Acute Lymphoblastic Leukaemia
11/01/2012 Post-ASH meeting 24
……inibs ?
Acute lymphoblastic leukemia: common emerging themes
• Very few lesions / case compared with AML
• Infant MLL R >> non-infant/adolescent ALL> adult ALL
• Structural rearrangements can be extremely complex at
molecular level : “chromotrypsis”
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Acute lymphoblastic leukemia: common emerging themes
• Very few lesions / case compared with AML
• Infant MLL R >> non-infant/adolescent ALL> adult ALL
• Structural rearrangements can be extremely complex at molecular
level : “chromotrypsis”
• Subclonal variation common at diagnosis, minor diagnostic subclone
can be origin of relapse
• Remarkable genetic heterogeneity among each of the subsets
analysed, but common themes can (sometimes) be identified
• BCR-ABL1-like ALL and potential targets for TKI
• ETP ALL resembling HSC rather than normal ETP : case for “myeloid”
induction therapy ?
11/01/2012 Post-ASH meeting 27
Post-ASH meeting 28 11/01/2012
Acute leukemia : 2012